Letter pubs.acs.org/OrgLett
Cite This: Org. Lett. 2018, 20, 1363−1366
Visible-Light-Induced External Radical-Triggered Annulation To Access CF2‑Containing Benzoxepine Derivatives Haoyue Xiang,† Qing-Lan Zhao,† Peng-Ju Xia,† Jun-An Xiao,‡ Zhi-Peng Ye,† Xiong Xie,† Huan Sheng,† Xiao-Qing Chen,*,† and Hua Yang*,† †
College of Chemistry and Chemical Engineering, Central South University, Changsha 410083, China College of Chemistry and Materials Science, Guangxi Teachers Education University, Nanning 530000, China
‡
S Supporting Information *
ABSTRACT: A facile and diversified synthesis of functionalized CF2-containing benzoxepine derivatives via photoredox catalysis was achieved in this work. This novel protocol features broad substrate scope, mild reaction conditions, operational simplicity, easy scale-up, and versatile derivatization, which would facilitate its practical and broad applications in the construction of valuable and synthetically challenging heterocycles.
B
emerged to rapidly install functionalized benzoxepines,4 which primarily relied on the metal-mediated cyclizations, such as palladium,4a rhodium,4d osmium,4e gold,4f and silver.4g Despite these impressive advances, in view of step-economy and green and sustainable chemistry, pursuing new annulation pathways accessing such valuable ring systems with higher bond-forming efficiency under mild conditions is of continued interest. Radical-triggered cascade reactions serve as ideal strategies in the synthesis of heterocyclic scaffolds, owing to multiple bonds which can be formed under a single set of reaction conditions. In recent years, photoredox catalysis has experienced a resurgence in interest as a powerful synthetic tool for effectively promoting radical-involved transformations.5 Particularly, the visible-lightinduced radical addition cascade annulation has demonstrated its synthetic utility in the construction of various ring systems6 but has rarely been extended to the assembly of a seven-membered cyclic system, especially benzoxepine. In a recent report describing photoredox catalytic cyclization of enaminones promoted by fluorinated radicals to synthesize fluorinated chromones,7 we demonstrated that the CC double bond in the enaminone motif showed an advantageous reactivity in the radical addition. Concurrently, the amino group acted as an excellent reductive quencher to regenerate the corresponding photocatalyst and drive the progress of the photocatalytic reaction while avoiding the need of adding stoichiometric reductants. We envisioned that merging an enaminone moiety with other functionality by rational design would provide a versatile photocatalytic platform in the assembly of challenging ring systems. Following this rationale, we intentionally preinstalled an enaminone moiety and olefin unit in the substrate
enzoxepines and their derivatives, as representative sevenmembered cyclic ethers, are widely encountered structural motifs in many natural products and pharmaceuticals1 (Figure 1)
Figure 1. Representative examples of important molecules containing a benzoxepine core skeleton.
with a variety of physiological and biological activities. Thus, development of efficient strategies to easily assemble this significant scaffold has received considerable attention. Unlike five- and six-membered cyclic ethers, the construction of seven-membered ethers may be more problematic due to unfavorable entropic penalties and transannular interactions associated with their formation.2 While challenging, the synthesis of benzoxepines has attracted intensive efforts to answer the needs of synthetic and medicinal chemistry. Generally, two major strategies accessing benzoxepines, intermolecular and intramolecular modes, predominately contributed to the progress of the methodology. A variety of transition-metal-catalyzed intermolecular [m + n]-cyclizations have been developed to construct this important heterocycle.3 Very recently, the groups of Jiang,3g Ren,3h and Meng3i reported base-mediated [4 + 3]annulation. Alternatively, various intramolecular annulations © 2018 American Chemical Society
Received: January 12, 2018 Published: February 15, 2018 1363
DOI: 10.1021/acs.orglett.8b00131 Org. Lett. 2018, 20, 1363−1366
Letter
Organic Letters Table 1. Investigation of Reaction Conditionsa
and thus designed novel precursors (E)-1-(2-(allyloxy)phenyl)3-(substituted amino)prop-2-en-1-ones 1 that can be readily synthesized from o-hydroxyacetophenones (Scheme 1). Scheme 1. Strategy Accessing Seven-Membered Cyclic Ethers
It was commonly accepted that the chemical and physical properties of heterocycles could be readily altered upon introduction of fluorinated functional groups, which is beneficial for modulating their biological activities.8 Given the recent success on the difunctionalization of alkenes9 and the significance of difluorinated analogues in medicinal chemistry, 2-bromo-2,2-difluoroacetic acid ethyl ester (BrCF2COOEt)10 could be considered an ideal fluorinated radical source. As part of our continued interest in the photoredox catalysis,7,11 we reasoned that simultaneous assembly of benzoxepines and installment of the CF2 unit can be easily realized under photocatalytic conditions (Scheme 1). We, herein, report a visible-light-driven external radical-triggered intramolecular annulation to efficiently assemble CF2-bearing benzoxepines, which would surely enrich the library of diverse fluorinecontaining seven-membered heterocycles. We commenced our exploration with the reaction of (E)-1-(2(allyloxy)phenyl)-3-(dimethylamino)prop-2-en-1-one (1a) with BrCF2COOEt (2) under irradiation of white LEDs (30 W) (Table 1). Catalyst screening demonstrated that Ir(dtbbpy)(bpy)2PF6 was the premium choice, whereas eosin Y and rhodamine B were ineffective in this reaction (Table 1, entries 1− 5). Noticeably, it was found that the enamine group was unexpectedly hydrolyzed, giving benzoxepine 3a bearing a 1,3dicarbonyl functional group as the corresponding enol. Conceivably, the resulting 1,3-dicarbonyl moiety offers broader synthetic opportunities for further derivatization of the resulting benzoxepines. Subsequently, several bases were also evaluated in the reaction, of which NaOAc provided the highest yield (Table 1, entries 6−10). In addition, various solvents were also screened (Table 1, entries 11−16), and CH2Cl2 was the optimal choice with a slightly improved yield (42%, Table 1, entry 14). Further increasing the amount of the catalyst did not improve the chemical yield (Table 1, entry 17). Because water is necessary for this transformation, 0.4 mL of H2O (CH2Cl2/H2O = 10:1) was added to this system, and desired product 3a was obtained in 57% yield. However, adding more water led to a slightly decreased yield. To gain mechanistic insight into the reaction, several control experiments were carried out. The desired product could not be obtained in the absence of photocatalyst or light (Table 1, entries 20 and 21), revealing that this transformation is a photocatalytic process. When TEMPO, as a radical inhibitor, was added into the reaction, no desired product was detected (Table 1, entry 22). This result indicates that a radical pathway may be involved in this transformation. To evaluate the substrate scope of this approach, various (E)1-(2-(allyloxy)phenyl)-3-(dimethylamino)prop-2-en-1-ones 1 were prepared and subjected to the optimized reaction conditions. As summarized in Scheme 2, the substitution patterns on the phenyl moiety were first modulated and
entry
catalyst
solvent
base
yieldb (%)
1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 18 19 20 21 22
eosin Y rhodamine B Ir(dtbbpy)(bpy)2PF6 Ir(ppy)3 Ru(bpy)3PF6 Ir(dtbbpy)(bpy)2PF6 Ir(dtbbpy)(bpy)2PF6 Ir(dtbbpy)(bpy)2PF6 Ir(dtbbpy)(bpy)2PF6 Ir(dtbbpy)(bpy)2PF6 Ir(dtbbpy)(bpy)2PF6 Ir(dtbbpy)(bpy)2PF6 Ir(dtbbpy)(bpy)2PF6 Ir(dtbbpy)(bpy)2PF6 Ir(dtbbpy)(bpy)2PF6 Ir(dtbbpy)(bpy)2PF6 Ir(dtbbpy)(bpy)2PF6 Ir(dtbbpy)(bpy)2PF6 Ir(dtbbpy)(bpy)2PF6
acetone acetone acetone acetone acetone acetone acetone acetone acetone acetone MeCN THF DCE CH2Cl2 DMF MeOH CH2Cl2 CH2Cl2 CH2Cl2 CH2Cl2 CH2Cl2 CH2Cl2
NaOAc NaOAc NaOAc NaOAc NaOAc
trace trace 30 18 12 15 18 trace trace